Analysis of the CYP21A2 gene pathogenic variants in CAH patients from Surgut using next-generation sequencing (NGS)

IF 1.2 Q4 GENETICS & HEREDITY Egyptian Journal of Medical Human Genetics Pub Date : 2024-03-12 DOI:10.1186/s43042-024-00502-9
Natalia Osinovskaya, Elena Vashukova, Olga Tarasenko, Maria Danilova, Olga Glavnova, Iskender Sultanov, Maxim Donnikov, Yulia Nasykhova, Andrey Glotov
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Abstract

21-hydroxylase deficiency is present in 90–95% of cases of congenital adrenal hyperplasia (CAH). Eleven major pathogenic variants account for 93% of all identified variants in the CYP21A2 gene in various clinical forms of the disease. Each population has its own range of significant pathogenic variants. We aimed to study the frequency of pathogenic variants in the CYP21A2 gene using NGS technology and real-time PCR in Surgut patients with different clinical forms of CAH. NGS was performed on 70 patients with salt-wasting and non-classical clinical forms of 21-hydroxylase deficiency, verified by direct Sanger sequencing and PCR–RFLP analysis. Eleven different pathogenic variants were found in 68.57% (48/70) of patients. Among 92.86% (13/14) of patients with salt-wasting CAH, variants were found to be homozygous, with CYP21A2 gene deletion as the most frequent mutation (46.4% or 13/28 alleles). In the group with non-classical CAH, pathogenic variants were identified only in 60.71% (34/56) of patients. V282L was discovered to be the most common variant in heterozygous carriers (45.45%, 15/33). NGS method identified 2 variants that were not determined by the standard method for major mutations detection: p.C170* and p.W22X, accounting for 3% of all known pathogenic variants. Our data make it possible to clarify the specific spectrum of CYP21A2 gene pathogenic variants in CAH patients from Surgut. The NGS method allows for the identification of rare pathogenic variants (3%) in the CYP21A2 gene that are not included in the conventional PCR–RFLP analysis.
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利用新一代测序技术(NGS)分析苏尔古特 CAH 患者的 CYP21A2 基因致病变体
在先天性肾上腺皮质增生症(CAH)的病例中,90%-95%存在 21-羟化酶缺乏症。在该病的各种临床形式中,CYP21A2 基因的 11 个主要致病变体占所有已发现变体的 93%。每个人群都有自己的重要致病变体。我们的目的是利用 NGS 技术和实时 PCR 研究不同临床形式 CAH 的 Surgut 患者中 CYP21A2 基因致病变异的频率。我们对 70 名患有盐耗竭和非典型临床形式 21- 羟化酶缺乏症的患者进行了 NGS,并通过直接 Sanger 测序和 PCR-RFLP 分析进行了验证。在 68.57%(48/70)的患者中发现了 11 种不同的致病变体。在92.86%(13/14)的盐耗竭型CAH患者中,变体均为同基因变异,其中CYP21A2基因缺失是最常见的变异(46.4%或13/28个等位基因)。在非典型 CAH 组中,仅在 60.71%(34/56)的患者中发现了致病变体。在杂合子携带者中,V282L 是最常见的变异(45.45%,15/33)。NGS 方法发现了 2 个主要变异检测标准方法无法确定的变异:p.C170* 和 p.W22X,占所有已知致病变异的 3%。我们的数据有助于明确苏尔古特 CAH 患者中 CYP21A2 基因致病变异的具体范围。NGS 方法可以鉴定出 CYP21A2 基因中罕见的致病变异(3%),而这些变异并不包括在传统的 PCR-RFLP 分析中。
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来源期刊
Egyptian Journal of Medical Human Genetics
Egyptian Journal of Medical Human Genetics Medicine-Genetics (clinical)
CiteScore
2.20
自引率
7.70%
发文量
150
审稿时长
18 weeks
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